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混杂 7TM 受体作为化学感受进食的新兴作用。

The emerging role of promiscuous 7TM receptors as chemosensors for food intake.

机构信息

Department of Medicinal Chemistry, Faculty of Pharmaceutical Sciences, University of Copenhagen, Copenhagen, Denmark.

出版信息

Vitam Horm. 2010;84:151-84. doi: 10.1016/B978-0-12-381517-0.00005-9.

DOI:10.1016/B978-0-12-381517-0.00005-9
PMID:21094899
Abstract

In recent years, several highly promiscuous seven transmembrane (7TM) receptors have been cloned and characterized of which many are activated broadly by amino acids, proteolytic degradation products, carbohydrates, or free fatty acids (FFAs) and are expressed in taste tissue, the gastrointestinal (GI) tract, endocrine glands, adipose tissue, and/or kidney. This has led to the hypothesis that these receptors may act as sensors of food intake modulating, for example, release of incretin hormones from the gut, insulin/glucagon from the pancreas, and leptin from adipose tissue. In the present review, we describe the molecular mechanisms of nutrient-sensing of the calcium-sensing receptor (CaR), the G protein-coupled receptor family C, group 6, subtype A (GPRC6A), and the taste1 receptor T1R1/T1R3-sensing L-α-amino acids; the carbohydrate-sensing T1R2/T1R3 receptor; the proteolytic degradation product sensor GPR93 (also termed GPR92); and the FFA sensing receptors FFA1, FFA2, FFA3, GPR84, and GPR120. Due to their omnipresent nature, the natural ligands have had limited usability in pharmacological/physiological studies which has hampered the elucidation of the physiological function and therapeutic prospect of their receptors. However, an increasing number of subtype-selective ligands and/or receptor knockout mice are being developed which at least for some of the receptors have validated them as promising drug targets in, for example, type II diabetes.

摘要

近年来,已经克隆和鉴定了几种高度混杂的七跨膜 (7TM) 受体,其中许多受体广泛被氨基酸、蛋白水解降解产物、碳水化合物或游离脂肪酸 (FFAs) 激活,并在味觉组织、胃肠道 (GI) 道、内分泌腺、脂肪组织和/或肾脏中表达。这导致了这样一种假设,即这些受体可能作为食物摄入的传感器,例如调节肠道中肠促胰岛素激素的释放、胰腺中的胰岛素/胰高血糖素和脂肪组织中的瘦素。在本综述中,我们描述了钙敏感受体 (CaR)、G 蛋白偶联受体家族 C、第 6 组、亚型 A (GPRC6A) 和味觉 1 受体 T1R1/T1R3 感知 L-α-氨基酸的营养感应的分子机制;碳水化合物感应 T1R2/T1R3 受体;蛋白水解降解产物传感器 GPR93(也称为 GPR92);以及 FFA 感应受体 FFA1、FFA2、FFA3、GPR84 和 GPR120。由于它们无处不在的性质,天然配体在药理学/生理学研究中的可用性有限,这阻碍了阐明其受体的生理功能和治疗前景。然而,越来越多的亚型选择性配体和/或受体敲除小鼠正在被开发出来,至少对于一些受体来说,它们已经被验证为 II 型糖尿病等疾病有前途的药物靶点。

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